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首页> 外文期刊>Melanoma research >Use of integrative epigenetic and cytogenetic analyses to identify novel tumor-suppressor genes in malignant melanoma.
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Use of integrative epigenetic and cytogenetic analyses to identify novel tumor-suppressor genes in malignant melanoma.

机译:利用综合表观遗传学和细胞遗传学分析来鉴定恶性黑色素瘤中的新型肿瘤抑制基因。

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摘要

The objective of this study was to identify novel tumor-suppressor genes in melanoma, using an integrative genomic approach. Data from: (i) earlier reports of DNA loss and gain in malignant melanoma accompanied by comparative genomic hybridization high-definition array data of the entire human genome; (ii) microarray expression data from melanoma-derived cell lines identifying genes with significantly increased expression due to methylation using a pharmacologic demethylating strategy; and (iii) publicly available RNA expression microarray data of primary tumors and benign nevi were integrated using statistical tools to define a population of candidate tumor-suppressor genes. Twenty-seven genes were identified in areas of deletion that demonstrated diminished expression in primary melanomas relative to benign nevi and were significantly increased in expression by 5-Aza treatment. Seven genes of these 27 genes demonstrated methylation and deletion in a validation cohort of 14 separate primary tumors. These were: CHRDL1, SFRP1, TMEM47, LPL, RARRES1, PLCXD1, and KOX15. All of these genes demonstrated growth-suppressive properties with transfection into melanoma-derived cell lines. Seven putative tumor-suppressor genes in malignant melanoma were identified using a novel integrative technique.
机译:这项研究的目的是使用综合基因组学方法鉴定黑色素瘤中的新型肿瘤抑制基因。来自以下方面的数据:(i)较早的恶性黑色素瘤DNA丢失和增加的报道,以及整个人类基因组的比较基因组杂交高清阵列数据; (ii)黑色素来源的细胞系的微阵列表达数据,使用药理学脱甲基化策略鉴定了由于甲基化而使表达显着增加的基因; (iii)使用统计工具整合原发性肿瘤和良性痣的可公开获得的RNA表达微阵列数据,以定义候选肿瘤抑制基因的种群。在缺失区域中鉴定出27个基因,这些基因显示了相对于良性痣在原发性黑色素瘤中表达减少,并通过5-Aza处理显着增加了表达。这27个基因中的7个基因在14个单独的原发性肿瘤的验证队列中显示出甲基化和缺失。它们是:CHRDL1,SFRP1,TMEM47,LPL,RARRES1,PLCXD1和KOX15。所有这些基因都具有转染到黑色素瘤来源的细胞系中的生长抑制特性。使用新型整合技术鉴定了恶性黑色素瘤中的七个推定的肿瘤抑制基因。

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